Department of Physiology and Pharmacology, University of Cantabria, Santander, Spain.
Cellular and Systems Neurobiology, Systems Biology Program, Centre for Genomic Regulation (CRG), Barcelona Institute of Science and Technology, Universitat Pompeu Fabra (UPF), Barcelona, Spain.
Prog Brain Res. 2020;251:245-268. doi: 10.1016/bs.pbr.2019.10.001. Epub 2019 Nov 1.
Neurodevelopmental disorders are challenging to study in the laboratory, and despite a large investment, few novel treatments have been developed in the last decade. While animal models have been valuable in elucidating disease mechanisms and in providing insights into the function of specific genes, the predictive validity of preclinical models to test potential therapies has been questioned. In the last two decades, diverse new murine models of Down syndrome (DS) have been developed and numerous studies have demonstrated neurobiological alterations that could be responsible for the cognitive and behavioral phenotypes found in this syndrome. In many cases, similar alterations were found in murine models and in individuals with DS, although several phenotypes shown in animals have yet not been confirmed in the human condition. Some of the neurobiological alterations observed in mice have been proposed to account for their changes in cognition and behavior, and have received special attention because of being putative therapeutic targets. Those include increased oxidative stress, altered neurogenesis, overexpression of the Dyrk1A gene, GABA-mediated overinhibition and Alzheimer's disease-related neurodegeneration. Subsequently, different laboratories have tested the efficacy of pharmacotherapies targeting these alterations. Unfortunately, animal models are limited in their ability to mimic the extremely complex process of human neurodevelopment and neuropathology. Therefore, the safety and efficacy identified in animal studies are not always translated to humans, and most of the drugs tested have not demonstrated any positive effect or very limited efficacy in clinical trials. Despite their limitations, though, animal trials give us extremely valuable information for developing and testing drugs for human use that cannot be obtained from molecular or cellular experiments alone. This chapter reviews some of these therapeutic approaches and discusses some reasons that could account for the discrepancy between the findings in mouse models of DS and in humans, including: (i) the incomplete resemble of the genetic alterations of available mouse models of DS and human trisomy 21, (ii) the lack of evidence that some of the phenotypic alterations found in mice (e.g., GABA-mediated overinhibition, and alterations in adult neurogenesis) are also present in DS individuals, and (iii) the inaccuracy and/or inadequacy of the methods used in clinical trials to detect changes in the cognitive and behavioral functions of people with DS. Despite the shortcomings of animal models, animal experimentation remains an invaluable tool in developing drugs. Thus, we will also discuss how to increase predictive validity of mouse models.
神经发育障碍在实验室中难以研究,尽管投入了大量资金,但在过去十年中仅开发出少数新的治疗方法。虽然动物模型在阐明疾病机制和深入了解特定基因的功能方面具有重要价值,但临床前模型预测潜在治疗方法的有效性一直受到质疑。在过去的二十年中,已经开发出多种新的唐氏综合征(DS)的小鼠模型,并且许多研究已经证明了神经生物学的改变,这些改变可能是导致该综合征认知和行为表型的原因。在许多情况下,在小鼠模型和患有 DS 的个体中都发现了类似的改变,尽管动物模型中表现出的一些表型尚未在人类疾病中得到证实。一些在小鼠中观察到的神经生物学改变被认为是其认知和行为改变的原因,并且由于它们是潜在的治疗靶点而受到特别关注。这些改变包括氧化应激增加、神经发生改变、Dyrk1A 基因过表达、GABA 介导的过度抑制和阿尔茨海默病相关的神经退行性变。随后,不同的实验室测试了针对这些改变的药物治疗的疗效。不幸的是,动物模型在模拟人类神经发育和神经病理学的极其复杂过程方面存在局限性。因此,在动物研究中确定的安全性和疗效并不总是能转化为人类,并且在临床试验中,大多数测试的药物都没有显示出任何积极效果或非常有限的疗效。尽管存在局限性,但动物试验为我们提供了开发和测试人类使用的药物的极其有价值的信息,这些信息无法仅从分子或细胞实验中获得。本章回顾了其中一些治疗方法,并讨论了一些导致 DS 小鼠模型和人类发现之间存在差异的原因,包括:(i)现有 DS 小鼠模型和人类 21 三体遗传改变的不完全相似性;(ii)缺乏证据表明在小鼠中发现的一些表型改变(例如 GABA 介导的过度抑制和成年神经发生的改变)也存在于 DS 个体中;以及(iii)临床试验中用于检测 DS 个体认知和行为功能变化的方法的不准确性和/或不充分性。尽管动物模型存在缺点,但动物实验仍然是开发药物的宝贵工具。因此,我们还将讨论如何提高小鼠模型的预测有效性。
